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O-Phenyl-3-iodotyramine

Chemical compound

Chemical compound

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o-Phenyl-3-iodotyramine (o-PIT) is a drug which acts as a selective agonist for the trace amine-associated receptor 1 (TAAR1). It has reasonable selectivity for TAAR1 but relatively low potency, and is rapidly metabolised in vivo, making it less useful for research than newer ligands such as RO5166017. Its values have been reported to be 35nM for the mouse TAAR1, 2.4nM at the rat TAAR1, and 9.5nM at the human TAAR1.

o-PIT has been found to produce effects in animals including hypothermia, hypolocomotion, antidepressant-like effects, anxiolytic-like effects, anti-obsessional-like effects, and antipsychotic-like effects, and inhibition of prepulse inhibition (PPI). These actions may be partially to fully dependent on TAAR1 agonism depending on the effect in question.

TAAR1 agonism has been implicated in modulating the effects of monoamine releasing agents (MRAs) like amphetamines. The MRA 3,4-methylenedioxymethamphetamine (MDMA) is a potent agonist of the mouse TAAR1, whereas the MRA para-chloroamphetamine (PCA) is not a significant agonist of the human TAAR1 or presumably of the mouse TAAR1. MDMA-induced in-vivo brain serotonin and dopamine release and hyperlocomotion are augmented in TAAR1 knockout mice relative to normal mice, whereas the in-vivo brain serotonin and dopamine release of PCA are not different between normal mice and TAAR1 knockout mice. In the same study, o-PIT blunted the dopamine and serotonin release of PCA in mouse synaptosomes in vitro, an effect that was absent in synaptosomes from TAAR1 knockout mice. These findings led to conclusions that TAAR1 agonism by MDMA auto-inhibits and constrains its own effects in rodents. Although MDMA is a potent TAAR1 agonist in rodents, it is a very weak and non-significant TAAR1 agonist in humans.

References

References

  1. (2022). "Regulation of Monoaminergic Functions by Gpcrs with a Special Emphasis on Mental and Movement Disorders".
  2. (December 2006). "Trace amine-associated receptors and their ligands". British Journal of Pharmacology.
  3. (July 2010). "Trace amines depress D(2)-autoreceptor-mediated responses on midbrain dopaminergic cells". British Journal of Pharmacology.
  4. (May 2011). "TAAR1 activation modulates monoaminergic neurotransmission, preventing hyperdopaminergic and hypoglutamatergic activity". Proceedings of the National Academy of Sciences of the United States of America.
  5. (February 2006). "Trace amine-associated receptor agonists: synthesis and evaluation of thyronamines and related analogues". J Med Chem.
  6. (August 2021). "Trace Amine-Associated Receptor 1 Contributes to Diverse Functional Actions of O-Phenyl-Iodotyramine in Mice but Not to the Effects of Monoamine-Based Antidepressants". Int J Mol Sci.
  7. (August 2015). "Trace amine-associated receptor 1: A promising target for the treatment of psychostimulant addiction". Eur J Pharmacol.
  8. (November 2011). "Genetic deletion of trace amine 1 receptors reveals their role in auto-inhibiting the actions of ecstasy (MDMA)". J Neurosci.
  9. (July 2018). "Trace Amines and Their Receptors". Pharmacol Rev.
  10. (2018). "Striatal Tyrosine Hydroxylase Is Stimulated via TAAR1 by 3-Iodothyronamine, But Not by Tyramine or β-Phenylethylamine". Front Pharmacol.
  11. (April 2016). "In Vitro Characterization of Psychoactive Substances at Rat, Mouse, and Human Trace Amine-Associated Receptor 1". J Pharmacol Exp Ther.
  12. (December 2011). "Trace amine-associated receptor 1 is a stereoselective binding site for compounds in the amphetamine class". Bioorganic & Medicinal Chemistry.
  13. (October 2018). "Dark Classics in Chemical Neuroscience: 3,4-Methylenedioxymethamphetamine". ACS Chem Neurosci.
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